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First-in-Class Chemical Probes against Poly(ADP-ribose) Glycohydrolase (PARG) Inhibit DNA Repair with Differential Pharmacology to Olaparib

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posted on 2016-09-30, 00:00 authored by Dominic I. James, Kate M. Smith, Allan M. Jordan, Emma E. Fairweather, Louise A. Griffiths, Nicola S. Hamilton, James R. Hitchin, Colin P. Hutton, Stuart Jones, Paul Kelly, Alison E. McGonagle, Helen Small, Alexandra I. J. Stowell, Julie Tucker, Ian D. Waddell, Bohdan Waszkowycz, Donald J. Ogilvie
The enzyme poly­(ADP-ribose) glycohydrolase (PARG) performs a critical role in the repair of DNA single strand breaks (SSBs). However, a detailed understanding of its mechanism of action has been hampered by a lack of credible, cell-active chemical probes. Herein, we demonstrate inhibition of PARG with a small molecule, leading to poly­(ADP-ribose) (PAR) chain persistence in intact cells. Moreover, we describe two advanced, and chemically distinct, cell-active tool compounds with convincing on-target pharmacology and selectivity. Using one of these tool compounds, we demonstrate pharmacology consistent with PARG inhibition. Further, while the roles of PARG and poly­(ADP-ribose) polymerase (PARP) are closely intertwined, we demonstrate that the pharmacology of a PARG inhibitor differs from that observed with the more thoroughly studied PARP inhibitor olaparib. We believe that these tools will facilitate a wider understanding of this important component of DNA repair and may enable the development of novel therapeutic agents exploiting the critical dependence of tumors on the DNA damage response (DDR).

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